Staging β -Amyloid Pathology with Amyloid Positron Emission Tomography

Mattsson, Niklas; Palmqvist, Sebastian; Stomrud, Erik; Vogel, Jacob; Hansson, Oskar

Staging β -Amyloid Pathology with Amyloid Positron Emission Tomography

Mark

Mattsson, Niklas ^LU

; Palmqvist, Sebastian ^LU

; Stomrud, Erik ^LU

; Vogel, Jacob and Hansson, Oskar ^LU

(2019) In JAMA Neurology 76(11). p.1319-1329

Abstract: Importance: Different brain regions appear to be involved during β-amyloid (Aβ) accumulation in Alzheimer disease (AD), but a longitudinally valid system to track Aβ stages in vivo using positron emission tomography (PET) is lacking. Objective: To construct a longitudinally valid in vivo staging system for AD using amyloid PET. Design, Setting, and Participants: Longitudinal multicenter cohort study using data accessed on August 20, 2018, from the Alzheimer's Disease Neuroimaging Initiative database of scans performed from June 9, 2010, to July 12, 2018, from 741 persons: 304 without cognitive impairment, 384 with mild cognitive impairment, and 53 with AD dementia. Cerebrospinal fluid (CSF) Aβ42 and fluorine 18-labeled florbetapir... (More); Importance: Different brain regions appear to be involved during β-amyloid (Aβ) accumulation in Alzheimer disease (AD), but a longitudinally valid system to track Aβ stages in vivo using positron emission tomography (PET) is lacking. Objective: To construct a longitudinally valid in vivo staging system for AD using amyloid PET. Design, Setting, and Participants: Longitudinal multicenter cohort study using data accessed on August 20, 2018, from the Alzheimer's Disease Neuroimaging Initiative database of scans performed from June 9, 2010, to July 12, 2018, from 741 persons: 304 without cognitive impairment, 384 with mild cognitive impairment, and 53 with AD dementia. Cerebrospinal fluid (CSF) Aβ42 and fluorine 18-labeled florbetapir (¹⁸F-florbetapir) data were used to determine early, intermediate, and late regions of Aβ accumulation. β-Amyloid stages ranging from 0 to 3 were constructed using these composites. Each subsequent stage required involvement of more advanced regions. Patients were followed up at 2, 4, and 6 years. Replication and validation were conducted using an independent cohort (Swedish BioFINDER) and gene expression information from the Allen Human Brain Atlas database. Analyses were conducted August 21, 2018, to May 24, 2019. Main Outcomes and Measures: The main outcome was change in stage. Stages were compared for diagnosis, CSF biomarkers of tau, and longitudinal atrophy, cognitive measures, and regional gene expression. Transitions between stages were tested using longitudinal ¹⁸F-florbetapir data. Results: Among 641 participants with CSF Aβ42 data and at least two ¹⁸F-florbetapir scans, 335 (52.3%) were male. The early region of Aβ accumulation included the precuneus, posterior cingulate, isthmus cingulate, insula, and medial and lateral orbitofrontal cortices. The late region included the lingual, pericalcarine, paracentral, precentral, and postcentral cortices. The intermediate region included remaining brain regions with increased accumulation rates. In 2072 PET scans from 741 participants, 2039 (98.4%) were unambiguously staged. At baseline, participants with stage 0 (n = 402) had a 14.7% (95% CI, 11.2%-18.1%) probability of progression to a higher stage; stage 1 (n = 21), 71.4% (95% CI, 50.0%-90.9%); and stage 2 (n = 79), 53.1% (95% CI, 42.2%-64.0%). Seven of the 741 participants (0.9%) reverted to a lower stage. Higher stages were associated with lower CSF Aβ42 concentrations (from stage 1 at baseline), greater CSF P-tau (from stage 1) and CSF T-tau (from stage 2), and accelerated cognitive decline (from stage 2) and atrophy (from stage 3), even when adjusting for clinical diagnosis. Key findings were replicated in the BioFINDER cohort (N = 474). The regions of different stages differed by gene expression profiles when using the transcriptome from the Allen Human Brain Atlas, especially involving genes associated with voltage-gated ion channel activity especially involving genes associated with voltage-gated ion channel activity, but also blood circulation, axon guidance, and lipid transportation. Conclusions and Relevance: Results of this study suggest that this robust staging system of Aβ accumulation may be useful for monitoring patients throughout the course of AD. Progression through stages may depend on underlying selective vulnerability in different brain regions.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/7ef820a6-b788-4660-887d-59239b9e0b73

author

Mattsson, Niklas ^LU

; Palmqvist, Sebastian ^LU

; Stomrud, Erik ^LU

; Vogel, Jacob and Hansson, Oskar ^LU

organization

publishing date

2019

type

Contribution to journal

publication status

published

subject

Neurology

in

JAMA Neurology

volume

76

issue

11

pages

11 pages

publisher

American Medical Association

external identifiers

pmid:31314895
scopus:85074813499

ISSN

2168-6149

DOI

10.1001/jamaneurol.2019.2214

language

English

LU publication?

yes

id

7ef820a6-b788-4660-887d-59239b9e0b73

date added to LUP

2019-11-29 13:52:34

date last changed

2024-04-17 00:33:31

@article{7ef820a6-b788-4660-887d-59239b9e0b73,
  abstract     = {{<p>Importance: Different brain regions appear to be involved during β-amyloid (Aβ) accumulation in Alzheimer disease (AD), but a longitudinally valid system to track Aβ stages in vivo using positron emission tomography (PET) is lacking. Objective: To construct a longitudinally valid in vivo staging system for AD using amyloid PET. Design, Setting, and Participants: Longitudinal multicenter cohort study using data accessed on August 20, 2018, from the Alzheimer's Disease Neuroimaging Initiative database of scans performed from June 9, 2010, to July 12, 2018, from 741 persons: 304 without cognitive impairment, 384 with mild cognitive impairment, and 53 with AD dementia. Cerebrospinal fluid (CSF) Aβ42 and fluorine 18-labeled florbetapir (<sup>18</sup>F-florbetapir) data were used to determine early, intermediate, and late regions of Aβ accumulation. β-Amyloid stages ranging from 0 to 3 were constructed using these composites. Each subsequent stage required involvement of more advanced regions. Patients were followed up at 2, 4, and 6 years. Replication and validation were conducted using an independent cohort (Swedish BioFINDER) and gene expression information from the Allen Human Brain Atlas database. Analyses were conducted August 21, 2018, to May 24, 2019. Main Outcomes and Measures: The main outcome was change in stage. Stages were compared for diagnosis, CSF biomarkers of tau, and longitudinal atrophy, cognitive measures, and regional gene expression. Transitions between stages were tested using longitudinal <sup>18</sup>F-florbetapir data. Results: Among 641 participants with CSF Aβ42 data and at least two <sup>18</sup>F-florbetapir scans, 335 (52.3%) were male. The early region of Aβ accumulation included the precuneus, posterior cingulate, isthmus cingulate, insula, and medial and lateral orbitofrontal cortices. The late region included the lingual, pericalcarine, paracentral, precentral, and postcentral cortices. The intermediate region included remaining brain regions with increased accumulation rates. In 2072 PET scans from 741 participants, 2039 (98.4%) were unambiguously staged. At baseline, participants with stage 0 (n = 402) had a 14.7% (95% CI, 11.2%-18.1%) probability of progression to a higher stage; stage 1 (n = 21), 71.4% (95% CI, 50.0%-90.9%); and stage 2 (n = 79), 53.1% (95% CI, 42.2%-64.0%). Seven of the 741 participants (0.9%) reverted to a lower stage. Higher stages were associated with lower CSF Aβ42 concentrations (from stage 1 at baseline), greater CSF P-tau (from stage 1) and CSF T-tau (from stage 2), and accelerated cognitive decline (from stage 2) and atrophy (from stage 3), even when adjusting for clinical diagnosis. Key findings were replicated in the BioFINDER cohort (N = 474). The regions of different stages differed by gene expression profiles when using the transcriptome from the Allen Human Brain Atlas, especially involving genes associated with voltage-gated ion channel activity especially involving genes associated with voltage-gated ion channel activity, but also blood circulation, axon guidance, and lipid transportation. Conclusions and Relevance: Results of this study suggest that this robust staging system of Aβ accumulation may be useful for monitoring patients throughout the course of AD. Progression through stages may depend on underlying selective vulnerability in different brain regions.</p>}},
  author       = {{Mattsson, Niklas and Palmqvist, Sebastian and Stomrud, Erik and Vogel, Jacob and Hansson, Oskar}},
  issn         = {{2168-6149}},
  language     = {{eng}},
  number       = {{11}},
  pages        = {{1319--1329}},
  publisher    = {{American Medical Association}},
  series       = {{JAMA Neurology}},
  title        = {{Staging β -Amyloid Pathology with Amyloid Positron Emission Tomography}},
  url          = {{http://dx.doi.org/10.1001/jamaneurol.2019.2214}},
  doi          = {{10.1001/jamaneurol.2019.2214}},
  volume       = {{76}},
  year         = {{2019}},
}

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Staging β -Amyloid Pathology with Amyloid Positron Emission Tomography